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在一个基于人群的队列中,酒精依赖的多基因风险与饮酒量、认知功能和社会剥夺相关。

Polygenic risk for alcohol dependence associates with alcohol consumption, cognitive function and social deprivation in a population-based cohort.

作者信息

Clarke Toni-Kim, Smith Andrew H, Gelernter Joel, Kranzler Henry R, Farrer Lindsay A, Hall Lynsey S, Fernandez-Pujals Ana M, MacIntyre Donald J, Smith Blair H, Hocking Lynne J, Padmanabhan Sandosh, Hayward Caroline, Thomson Pippa A, Porteous David J, Deary Ian J, McIntosh Andrew M

机构信息

Division of Psychiatry.

Division of Human Genetics, Department of Psychiatry, Yale University School of Medicine, VA CT Healthcare Center, West Haven, CT, USA.

出版信息

Addict Biol. 2016 Mar;21(2):469-80. doi: 10.1111/adb.12245. Epub 2015 Apr 10.

Abstract

Alcohol dependence is frequently co-morbid with cognitive impairment. The relationship between these traits is complex as cognitive dysfunction may arise as a consequence of heavy drinking or exist prior to the onset of dependence. In the present study, we tested the genetic overlap between cognitive abilities and alcohol dependence using polygenic risk scores (PGRS). We created two independent PGRS derived from two recent genome-wide association studies (GWAS) of alcohol dependence (SAGE GWAS: n = 2750; Yale-Penn GWAS: n = 2377) in a population-based cohort, Generation Scotland: Scottish Family Health Study (GS:SFHS) (n = 9863). Data on alcohol consumption and four tests of cognitive function [Mill Hill Vocabulary (MHV), digit symbol coding, phonemic verbal fluency (VF) and logical memory] were available. PGRS for alcohol dependence were negatively associated with two measures of cognitive function: MHV (SAGE: P = 0.009, β = -0.027; Yale-Penn: P = 0.001, β = -0.034) and VF (SAGE: P = 0.0008, β = -0.036; Yale-Penn: P = 0.00005, β = -0.044). VF remained robustly associated after adjustment for education and social deprivation; however, the association with MHV was substantially attenuated. Shared genetic variants may account for some of the phenotypic association between cognitive ability and alcohol dependence. A significant negative association between PGRS and social deprivation was found (SAGE: P = 5.2 × 10(-7) , β = -0.054; Yale-Penn: P = 0.000012, β = -0.047). Individuals living in socially deprived regions were found to carry more alcohol dependence risk alleles which may contribute to the increased prevalence of problem drinking in regions of deprivation. Future work to identify genes which affect both cognitive impairment and alcohol dependence will help elucidate biological processes common to both disorders.

摘要

酒精依赖常与认知障碍共病。这些特征之间的关系很复杂,因为认知功能障碍可能是大量饮酒的结果,也可能在依赖开始之前就已存在。在本研究中,我们使用多基因风险评分(PGRS)测试了认知能力与酒精依赖之间的遗传重叠。我们在一个基于人群的队列——苏格兰一代:苏格兰家庭健康研究(GS:SFHS)(n = 9863)中,从两项最近的酒精依赖全基因组关联研究(GWAS)(SAGE GWAS:n = 2750;耶鲁 - 宾夕法尼亚GWAS:n = 2377)中创建了两个独立的PGRS。有关于酒精消费和四项认知功能测试的数据[米尔希尔词汇(MHV)、数字符号编码、音素言语流畅性(VF)和逻辑记忆]。酒精依赖的PGRS与两项认知功能指标呈负相关:MHV(SAGE:P = 0.009,β = -0.027;耶鲁 - 宾夕法尼亚:P = 0.001,β = -0.034)和VF(SAGE:P = 0.0008,β = -0.036;耶鲁 - 宾夕法尼亚:P = 0.00005,β = -0.044)。在调整教育和社会剥夺因素后,VF仍具有显著相关性;然而,与MHV的关联大幅减弱。共享的基因变异可能解释了认知能力与酒精依赖之间的一些表型关联。发现PGRS与社会剥夺之间存在显著负相关(SAGE:P = 5.2 × 10⁻⁷,β = -0.054;耶鲁 - 宾夕法尼亚:P = 0.000012,β = -0.047)。生活在社会剥夺地区的个体被发现携带更多酒精依赖风险等位基因,这可能导致贫困地区问题饮酒患病率增加。未来识别影响认知障碍和酒精依赖的基因的工作将有助于阐明这两种疾病共有的生物学过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d71/4863720/576cce0f00c6/ADB-21-469-g001.jpg

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